| Literature DB >> 30918406 |
David Zeevi1,2,3, Tal Korem4,5,6,7, Anastasia Godneva4,5, Noam Bar4,5, Alexander Kurilshikov8, Maya Lotan-Pompan4,5, Adina Weinberger4,5, Jingyuan Fu8,9, Cisca Wijmenga8,10, Alexandra Zhernakova8, Eran Segal11,12.
Abstract
Differences in the presence of even a few genes between otherwise identical bacterial strains may result in critical phenotypic differences. Here we systematically identify microbial genomic structural variants (SVs) and find them to be prevalent in the human gut microbiome across phyla and to replicate in different cohorts. SVs are enriched for CRISPR-associated and antibiotic-producing functions and depleted from housekeeping genes, suggesting that they have a role in microbial adaptation. We find multiple associations between SVs and host disease risk factors, many of which replicate in an independent cohort. Exploring genes that are clustered in the same SV, we uncover several possible mechanistic links between the microbiome and its host, including a region in Anaerostipes hadrus that encodes a composite inositol catabolism-butyrate biosynthesis pathway, the presence of which is associated with lower host metabolic disease risk. Overall, our results uncover a nascent layer of variability in the microbiome that is associated with microbial adaptation and host health.Entities:
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Year: 2019 PMID: 30918406 DOI: 10.1038/s41586-019-1065-y
Source DB: PubMed Journal: Nature ISSN: 0028-0836 Impact factor: 49.962